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Genomic Profiling of Biliary Tract Cancer Cell Lines Reveals Molecular Subtypes and Actionable Drug Targets

机译:胆道癌细胞系的基因组分析显示分子亚型和可操作的药物靶标

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摘要

Summary: Biliary tract cancers (BTCs) currently have no approved targeted therapies. Although genomic profiling of primary BTCs has identified multiple potential drug targets, accurate models are needed for their evaluation. Genomic profiling of 22 BTC cell lines revealed they harbor similar mutational signatures, recurrently mutated genes, and genomic alterations to primary tumors. Transcriptomic profiling identified two major subtypes, enriched for epithelial and mesenchymal genes, which were also evident in patient-derived organoids and primary tumors. Interrogating these models revealed multiple mechanisms of MAPK signaling activation in BTC, including co-occurrence of low-activity BRAF and MEK mutations with receptor tyrosine kinase overexpression. Finally, BTC cell lines with altered ERBB2 or FGFRs were exquisitely sensitive to specific targeted agents, whereas surprisingly, IDH1-mutant lines did not respond to IDH1 inhibitors in vitro. These findings establish BTC cell lines as robust models of primary disease, reveal specific molecular disease subsets, and highlight specific molecular vulnerabilities in these cancers. : Biological Sciences; Genetics; Genomics; Cancer Subject Areas: Biological Sciences, Genetics, Genomics, Cancer
机译:摘要:胆道癌(BTCS),目前还没有批准的靶向疗法。虽然主要BTCS的基因组分析已确定多个潜在的药物靶点,需要对自己的评价精确的模型。的22家BTC细胞系的基因组谱显示它们怀有类似突变签名,反复突变的基因,和基因组改变到原发肿瘤。转录纹确定了两个主要的亚型,富集了上皮细胞和间充质的基因,这也很明显在患者来源的类器官和原发性肿瘤。询问这些模型揭示了BTC MAPK信号传导激活的多种机制,包括低活性BRAF和MEK突变的同现与受体酪氨酸激酶的过度表达。最后,具有改变的或ERBB2的FGFR BTC细胞系对特定靶向药物非常敏感,而令人惊奇地,IDH1突变的线没有在体外IDH1抑制剂响应。这些研究结果建立BTC细胞系原发疾病的可靠的模型,揭示了特定的分子病子集,并在这些癌症突出显示特定分子的漏洞。 : 生物科学;遗传学;基因组学;巨蟹座学科领域:生命科学,遗传学,基因组学,癌症

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